Muscle Damage in Dystrophic mdx Mice Is Influenced by the Activity of Ca(2+)-Activated K(Ca)3.1 Channels

Duchenne muscular dystrophy (DMD) is an X-linked disease, caused by a mutant dystrophin gene, leading to muscle membrane instability, followed by muscle inflammation, infiltration of pro-inflammatory macrophages and fibrosis. The calcium-activated potassium channel type 3.1 (K(Ca)3.1) plays key role...

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Autores principales: Morotti, Marta, Garofalo, Stefano, Cocozza, Germana, Antonangeli, Fabrizio, Bianconi, Valeria, Mozzetta, Chiara, De Stefano, Maria Egle, Capitani, Riccardo, Wulff, Heike, Limatola, Cristina, Catalano, Myriam, Grassi, Francesca
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2022
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9025295/
https://www.ncbi.nlm.nih.gov/pubmed/35455028
http://dx.doi.org/10.3390/life12040538
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author Morotti, Marta
Garofalo, Stefano
Cocozza, Germana
Antonangeli, Fabrizio
Bianconi, Valeria
Mozzetta, Chiara
De Stefano, Maria Egle
Capitani, Riccardo
Wulff, Heike
Limatola, Cristina
Catalano, Myriam
Grassi, Francesca
author_facet Morotti, Marta
Garofalo, Stefano
Cocozza, Germana
Antonangeli, Fabrizio
Bianconi, Valeria
Mozzetta, Chiara
De Stefano, Maria Egle
Capitani, Riccardo
Wulff, Heike
Limatola, Cristina
Catalano, Myriam
Grassi, Francesca
author_sort Morotti, Marta
collection PubMed
description Duchenne muscular dystrophy (DMD) is an X-linked disease, caused by a mutant dystrophin gene, leading to muscle membrane instability, followed by muscle inflammation, infiltration of pro-inflammatory macrophages and fibrosis. The calcium-activated potassium channel type 3.1 (K(Ca)3.1) plays key roles in controlling both macrophage phenotype and fibroblast proliferation, two critical contributors to muscle damage. In this work, we demonstrate that pharmacological blockade of the channel in the mdx mouse model during the early degenerative phase favors the acquisition of an anti-inflammatory phenotype by tissue macrophages and reduces collagen deposition in muscles, with a concomitant reduction of muscle damage. As already observed with other treatments, no improvement in muscle performance was observed in vivo. In conclusion, this work supports the idea that K(Ca)3.1 channels play a contributing role in controlling damage-causing cells in DMD. A more complete understanding of their function could lead to the identification of novel therapeutic approaches.
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spelling pubmed-90252952022-04-23 Muscle Damage in Dystrophic mdx Mice Is Influenced by the Activity of Ca(2+)-Activated K(Ca)3.1 Channels Morotti, Marta Garofalo, Stefano Cocozza, Germana Antonangeli, Fabrizio Bianconi, Valeria Mozzetta, Chiara De Stefano, Maria Egle Capitani, Riccardo Wulff, Heike Limatola, Cristina Catalano, Myriam Grassi, Francesca Life (Basel) Article Duchenne muscular dystrophy (DMD) is an X-linked disease, caused by a mutant dystrophin gene, leading to muscle membrane instability, followed by muscle inflammation, infiltration of pro-inflammatory macrophages and fibrosis. The calcium-activated potassium channel type 3.1 (K(Ca)3.1) plays key roles in controlling both macrophage phenotype and fibroblast proliferation, two critical contributors to muscle damage. In this work, we demonstrate that pharmacological blockade of the channel in the mdx mouse model during the early degenerative phase favors the acquisition of an anti-inflammatory phenotype by tissue macrophages and reduces collagen deposition in muscles, with a concomitant reduction of muscle damage. As already observed with other treatments, no improvement in muscle performance was observed in vivo. In conclusion, this work supports the idea that K(Ca)3.1 channels play a contributing role in controlling damage-causing cells in DMD. A more complete understanding of their function could lead to the identification of novel therapeutic approaches. MDPI 2022-04-05 /pmc/articles/PMC9025295/ /pubmed/35455028 http://dx.doi.org/10.3390/life12040538 Text en © 2022 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Morotti, Marta
Garofalo, Stefano
Cocozza, Germana
Antonangeli, Fabrizio
Bianconi, Valeria
Mozzetta, Chiara
De Stefano, Maria Egle
Capitani, Riccardo
Wulff, Heike
Limatola, Cristina
Catalano, Myriam
Grassi, Francesca
Muscle Damage in Dystrophic mdx Mice Is Influenced by the Activity of Ca(2+)-Activated K(Ca)3.1 Channels
title Muscle Damage in Dystrophic mdx Mice Is Influenced by the Activity of Ca(2+)-Activated K(Ca)3.1 Channels
title_full Muscle Damage in Dystrophic mdx Mice Is Influenced by the Activity of Ca(2+)-Activated K(Ca)3.1 Channels
title_fullStr Muscle Damage in Dystrophic mdx Mice Is Influenced by the Activity of Ca(2+)-Activated K(Ca)3.1 Channels
title_full_unstemmed Muscle Damage in Dystrophic mdx Mice Is Influenced by the Activity of Ca(2+)-Activated K(Ca)3.1 Channels
title_short Muscle Damage in Dystrophic mdx Mice Is Influenced by the Activity of Ca(2+)-Activated K(Ca)3.1 Channels
title_sort muscle damage in dystrophic mdx mice is influenced by the activity of ca(2+)-activated k(ca)3.1 channels
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9025295/
https://www.ncbi.nlm.nih.gov/pubmed/35455028
http://dx.doi.org/10.3390/life12040538
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